Application is based on
randomized, controlled and long-term extension
data for leniolisib as a treatment for APDS, a rare primary
immunodeficiency
This submission follows the grant of
accelerated assessment allowing an expedited review for leniolisib
from a standard 210 days to 150 days
LEIDEN, Netherlands, Oct. 11,
2022 /PRNewswire/ -- Pharming Group N.V. ("Pharming"
or "the Company") (EURONEXT Amsterdam: PHARM/Nasdaq: PHAR)
announces that it has submitted a Marketing Authorisation
Application (MAA) to the European Medicines Agency (EMA) for
leniolisib, an oral, selective phosphoinositide 3-kinase delta
(PI3Kδ) inhibitor, as a treatment for activated phosphoinositide
3-kinase delta syndrome (APDS), a rare primary immunodeficiency, in
adults and adolescents 12 years or older.
On August 1, 2022, Pharming
announced the leniolisib MAA was granted accelerated assessment by
EMA's Committee for Medicinal Products for Human Use (CHMP). The
accelerated assessment reduces the review timeframe from 210 days
to 150 days. Upon request, the EMA will grant an accelerated
assessment of an MAA if they decide the product is of major
interest for public health, and in particular, from the viewpoint
of therapeutic innovation. Marketing authorisation for
leniolisib in the EEA is anticipated in H1 2023.
Anurag Relan, Chief Medical
Officer of Pharming, commented:
"This MAA submission, under an accelerated regulatory
pathway, is an important step towards approval of our second
product in the EEA and highlights Pharming's ongoing commitment to
advancing leniolisib as a treatment for patients with APDS. There
is a significant unmet need for therapies to improve outcomes for
these patients, which, if left untreated, can result in permanent
lung damage and lymphoma. Leniolisib has the potential to be the
first approved treatment for this rare and orphan-designated
disease, and we look forward to continuing our work with key
stakeholders to bring this new product to patients."
The MAA is supported by positive data from a Phase II/III study
of leniolisib, announced on February 2,
2022, which met its co-primary endpoints of reduction in
lymph node size and correction of immunodeficiency in the target
population. Furthermore, safety data from the study showed that
leniolisib was well tolerated by participants. Also submitted as
part of the MAA were data from a long-term, open-label extension
clinical trial in patients with APDS treated with leniolisib.
About Activated Phosphoinositide
3-Kinase δ Syndrome (APDS)
APDS is a rare primary immunodeficiency that affects
approximately 1 to 2 people per million. It is caused by variants
in either of two
genes, PIK3CD or PIK3R1, that regulate
maturation of white blood cells. Variants of these genes lead to
hyperactivity of the PI3Kδ (phosphoinositide 3-kinase delta)
pathway.1,2 Balanced signaling in the PI3Kδ pathway
is essential for physiological immune function. When this pathway
is hyperactive, immune cells fail to mature and function properly,
leading to immunodeficiency and
dysregulation.1,3 APDS is characterized by severe,
recurrent sinopulmonary infections, lymphoproliferation,
autoimmunity, and enteropathy.4,5 Because these
symptoms can be associated with a variety of conditions, including
other primary immunodeficiencies, people with APDS are frequently
misdiagnosed and suffer a median 7-year diagnostic
delay.6 As APDS is a progressive disease, this
delay may lead to an accumulation of damage over time, including
permanent lung damage and lymphoma.4-7 The only way
to definitively diagnose this condition is through genetic
testing.
About Leniolisib
Leniolisib is a small-molecule inhibitor of the delta isoform of
the 110 kDa catalytic subunit of class IA PI3K with
immunomodulating and potentially anti-neoplastic activities.
Leniolisib inhibits the production of
phosphatidylinositol-3-4-5-trisphosphate (PIP3). PIP3 serves as an
important cellular messenger activating AKT (via PDK1) and
regulates a multitude of cell functions such as proliferation,
differentiation, cytokine production, cell survival, angiogenesis,
and metabolism. Unlike PI3Kα and PI3Kβ, which are ubiquitously
expressed, PI3Kẟ and PI3Kγ are expressed primarily in cells of
hematopoietic origin. The central role of PI3Kẟ in regulating
numerous cellular functions of the adaptive immune system (B-cells
and, to a lesser extent, T cells) as well as the innate immune
system (neutrophils, mast cells, and macrophages) strongly
indicates that PI3Kẟ is a valid and potentially effective
therapeutic target for several immune diseases. To date, leniolisib
has been well tolerated during both the Phase 1 first-in-human
trial in healthy subjects and the Phase II/III
registration-enabling study.
About Pharming Group N.V.
Pharming Group N.V. (Euronext Amsterdam: PHARM)
(NASDAQ: PHAR) is a global biopharmaceutical company dedicated
to transforming the lives of patients with rare, debilitating, and
life-threatening diseases. Pharming is commercializing and
developing an innovative portfolio of protein replacement therapies
and precision medicines, including small molecules, biologics, and
gene therapies that are in early to late-stage development.
Pharming is headquartered in Leiden, Netherlands, and has
employees around the globe who serve patients in over 30 markets
in North America, Europe, the Middle
East, Africa, and Asia-Pacific.
For more information, visit www.pharming.com and find
us on LinkedIn
Forward-Looking Statements
This press release contains forward-looking statements,
including with respect to timing and progress of Pharming's
preclinical studies and clinical trials of its product candidates,
Pharming's clinical and commercial prospects, Pharming's ability to
overcome the challenges posed by the COVID-19 pandemic to the
conduct of its business, and Pharming's expectations regarding its
projected working capital requirements and cash resources, which
statements are subject to a number of risks, uncertainties and
assumptions, including, but not limited to the scope, progress and
expansion of Pharming's clinical trials and ramifications for the
cost thereof; and clinical, scientific, regulatory and technical
developments. In light of these risks and uncertainties, and other
risks and uncertainties that are described in Pharming's 2021
Annual Report and the Annual Report on Form 20-F for the year
ended December 31, 2021 filed with the U.S. Securities
and Exchange Commission, the events and circumstances discussed in
such forward-looking statements may not occur, and Pharming's
actual results could differ materially and adversely from those
anticipated or implied thereby. Any forward-looking statements
speak only as of the date of this press release and are based on
information available to Pharming as of the date of this
release.
Inside Information
This press release relates to the disclosure of information
that qualifies, or may have qualified, as inside information within
the meaning of Article 7(1) of the EU Market Abuse
Regulation.
References
- Lucas CL, et al. Nat Immunol. 2014;15:88-97.
- Elkaim E, et al. J Allergy Clin
Immunol. 2016;138(1):210-218.
- Nunes-Santos
C, Uzel G, Rosenzweig SD. J Allergy Clin
Immunol. 2019;143(5):1676-1687.
- Coulter TI, et al. J Allergy Clin Immunol.
2017;139(2):597-606.
- Maccari ME, et al. Front Immunol.
2018;9:543.
- Jamee M, et al. Clin Rev
Allergy Immunol. 2019;May
21.
- Condliffe AM, Chandra A. Front Immunol.
2018;9:338.
For further public information, contact:
Pharming Group, Leiden, The Netherlands
Heather
Robertson, Investor Relations & Corporate Communications
Manager
T: +31 71 524 7400
E: investor@pharming.com
FTI Consulting, London, UK
Victoria Foster Mitchell/Alex Shaw/Amy
Byrne
T: +44 203 727 1000
LifeSpring Life Sciences Communication, Amsterdam,
The Netherlands
Leon
Melens
T: +31 6 53 81 64 27
E: pharming@lifespring.nl
US PR:
Ethan
Metelenis
T: +1 (917) 882 9038
E: Ethan.Metelenis@precisionvh.com
EU PR:
Dan Caley
T: +44 (0) 787 546 8942
E: Dan.caley@aprilsix.com
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SOURCE Pharming Group N.V.